Abstract

BackgroundResponding emotionally to danger is critical for survival. Normal functioning also requires flexible alteration of emotional responses when a threat becomes safe. Aberrant threat and safety learning occur in many psychiatric disorders, including posttraumatic stress disorder, obsessive-compulsive disorder, and schizophrenia, in which emotional responses can persist pathologically. While there is evidence that threat and safety learning can be modulated by the serotonin systems, there have been few studies in humans. We addressed a critical clinically relevant question: How does lowering serotonin affect memory retention of conditioned threat and safety memory? MethodsForty-seven healthy participants underwent conditioning to two stimuli predictive of threat on day 1. One stimulus but not the other was subsequently presented in an extinction session. Emotional responding was assessed by the skin conductance response. On day 2, we employed acute dietary tryptophan depletion to lower serotonin temporarily, in a double-blind, placebo-controlled, randomized between-groups design. We then tested for the retention of conditioned threat and extinction memory. We also measured self-reported intolerance of uncertainty, known to modulate threat memory expression. ResultsThe expression of emotional memory was attenuated in participants who had undergone tryptophan depletion. Individuals who were more intolerant of uncertainty showed even greater attenuation of emotion following depletion. ConclusionsThese results support the view that serotonin is involved in predicting aversive outcomes and refine our understanding of the role of serotonin in the persistence of emotional responsivity, with implications for individual differences in vulnerability to psychopathology.

Highlights

  • Responding emotionally to danger is critical for survival

  • Repeated-measures analysis of covariance (ANCOVA) with group assignment and sex as between-subjects factors, stimulus (CS1E, CS1N, CS2; all trials) as a within-subjects factor, and Intolerance of Uncertainty Scale (IUS) as a covariate yielded a main effect of stimulus (F1,56 = 9.239, p = .002, hp2 = .180), no main effect of group assignment (F1,42 = 0.591, p = .446, hp2 = .014), and no group assignment 3 stimulus interaction (F1,56 = 1.272, p = .277, hp2 = .029)

  • The key result was that Acute tryptophan depletion (ATD) attenuated the expression of previously acquired emotion in the spontaneous recovery phase

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Summary

Introduction

Responding emotionally to danger is critical for survival. Normal functioning requires flexible alteration of emotional responses when a threat becomes safe. We addressed a critical clinically relevant question: How does lowering serotonin affect memory retention of conditioned threat and safety memory? On day 2, we employed acute dietary tryptophan depletion to lower serotonin temporarily, in a double-blind, placebo-controlled, randomized between-groups design. We tested for the retention of conditioned threat and extinction memory. We measured self-reported intolerance of uncertainty, known to modulate threat memory expression. RESULTS: The expression of emotional memory was attenuated in participants who had undergone tryptophan depletion. Individuals who were more intolerant of uncertainty showed even greater attenuation of emotion following depletion. CONCLUSIONS: These results support the view that serotonin is involved in predicting aversive outcomes and refine our understanding of the role of serotonin in the persistence of emotional responsivity, with implications for individual differences in vulnerability to psychopathology

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